Schwager Samantha C, Mosier Jenna A, Padmanabhan Reethi S, White Addison, Xing Qinzhe, Hapach Lauren A, Taufalele Paul V, Ortiz Ismael, Reinhart-King Cynthia A
Department of Biomedical Engineering, Vanderbilt University, Nashville, TN 37212 USA.
Nancy E. and Peter C. Meinig School of Biomedical Engineering, Cornell University, Ithaca, NY 14853, USA.
iScience. 2022 Oct 1;25(10):105190. doi: 10.1016/j.isci.2022.105190. eCollection 2022 Oct 21.
Intracellular and environmental cues result in heterogeneous cancer cell populations with different metabolic and migratory behaviors. Although glucose metabolism and epithelial-to-mesenchymal transition have previously been linked, we aim to understand how this relationship fuels cancer cell migration. We show that while glycolysis drives single-cell migration in confining microtracks, fast and slow cells display different migratory sensitivities to glycolysis and oxidative phosphorylation inhibition. Phenotypic sorting of highly and weakly migratory subpopulations (MDA, MDA) reveals that more mesenchymal, highly migratory MDA preferentially use glycolysis while more epithelial, weakly migratory MDA utilize mitochondrial respiration. These phenotypes are plastic and MDA can be made less glycolytic, mesenchymal, and migratory and MDA can be made more glycolytic, mesenchymal, and migratory via modulation of glucose metabolism or EMT. These findings reveal an intrinsic link between EMT and glucose metabolism that controls migration. Identifying mechanisms fueling phenotypic heterogeneity is essential to develop targeted metastatic therapeutics.
细胞内和环境信号导致具有不同代谢和迁移行为的异质性癌细胞群体。尽管葡萄糖代谢与上皮-间质转化此前已有关联,但我们旨在了解这种关系如何促进癌细胞迁移。我们发现,虽然糖酵解驱动癌细胞在狭窄微通道中的单细胞迁移,但快速迁移和缓慢迁移的细胞对糖酵解和氧化磷酸化抑制表现出不同的迁移敏感性。对高迁移性和低迁移性亚群(MDA、MDA)进行表型分选后发现,更具间充质特征、高迁移性的MDA优先利用糖酵解,而更具上皮特征、低迁移性的MDA则利用线粒体呼吸。这些表型具有可塑性,通过调节葡萄糖代谢或上皮-间质转化,MDA可以减少糖酵解、间充质特征和迁移能力,而MDA可以增加糖酵解、间充质特征和迁移能力。这些发现揭示了上皮-间质转化与控制迁移的葡萄糖代谢之间的内在联系。确定导致表型异质性的机制对于开发靶向转移性治疗至关重要。
Zotero 插件
